Palladium-Catalyzed Amination of Unprotected Halo-7-azaindoles

Sep 22, 2010 - Joseph P. Tassone , Preston M. MacQueen , Christopher M. Lavoie , Michael J. Ferguson , Robert McDonald , and Mark Stradiotto...
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ORGANIC LETTERS

Palladium-Catalyzed Amination of Unprotected Halo-7-azaindoles

2010 Vol. 12, No. 20 4438-4441

Jaclyn L. Henderson, Sarah M. McDermott, and Stephen L. Buchwald* Department of Chemistry, Room 18-490, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, United States [email protected] Received August 16, 2010

ABSTRACT

Simple and efficient procedures for the Pd-catalyzed cross-coupling of primary and secondary amines with halo-7-azaindoles(pyrrolo[2,3b]pyridine) are presented. Previously, no general method was available to ensure the highly selective reaction of the heteroaryl halide in the presence of the unprotected azaindole N-H. Using palladium precatalysts recently reported by our group, such reactions are easily accomplished under mild conditions that can be applied to cross-coupling reactions with a wide array of aliphatic and aromatic amines.

Azaindoles have been receiving increased attention from the pharmaceutical and agrochemical industries over the past decade, due both to their potential as indole-isosteres and as interesting core structures in their own right.1,2 The substitution of a carbon by a nitrogen not only confers altered electronic properties but also adds a potential hydrogen bond acceptor, which can form the basis for altering the physicochemical or biological properties of a compound.3 The close proximity of hydrogen bond donor and acceptor sites also distinguishes azaindoles as important substructures in dyes, ligands for transition metals, and novel materials.2,4 Despite their utility, methods for the synthesis and functionalization of azaindole scaffolds remain limited. The majority of methods provide N-1, C-2, or C-3 substituted structures, with few offering general solutions to functionalization of the pyridine ring.2,5-7 A particularly interesting subset of these molecules are amino-substituted azaindoles, (1) Lednicer, D. Strategies for Organic Drug Synthesis and Design, 2nd ed.; Wiley: Hoboken, 2009. (2) Popowycz, F.; Routier, S.; Joseph, B.; Merour, J. Y. Tetrahedron 2007, 63, 1031–1064. (3) Kulagowski, J. J.; Broughton, H. B.; Curtis, N. R.; Mawer, I. M.; Ridgill, M. P.; Baker, R.; Emms, F.; Freedman, S. B.; Marwood, R.; Patel, S.; Ragan, C. I.; Leeson, P. D. J. Med. Chem. 1996, 39, 1941–1942. (4) Hudson, Z. M.; Wang, S. Acc. Chem. Res. 2009, 42, 1584–1596. (5) Merour, J. Y.; Joseph, B. Curr. Org. Chem. 2001, 5, 471–506. (6) Song, J. J.; Reeves, J. T.; Gallou, F.; Tan, Z. L.; Yee, N. K.; Senanayake, C. H. Chem. Soc. ReV. 2007, 36, 1120–1132. (7) Prokopov, A. A.; Yakhontov, L. N. Pharm. Chem. J. 1994, 28, 30– 51. 10.1021/ol101928m  2010 American Chemical Society Published on Web 09/22/2010

which appear in a variety of biologically active molecules (Figure 1)8-12 and can be particularly challenging or lengthy to prepare Via reported methods. Amino-7-azaindoles are often accessed from the corresponding halide Via SNAr displacement reactions, which typically require high temperatures, extended reaction times, and a large excess of the amine partner.13 Furthermore, 5-haloazaindoles are not suitable substrates for SNAr, nor are some amines. Alternative approaches employ the amino-substituted azaindole as the key intermediate, which can be challenging to prepare.14 Our approach to the synthesis of amino-azaindoles is to use Pd-mediated cross-coupling technology15-18 for the (8) Blake, J.; Gunawardana, I. W.; Le, H. Y.; Mohr, P. J.; Wallace, E. M.; Wang, B. Pyrrolo[2,3-b]pyridines as CHK1 and CHK2 kinase inhibitors for the treatment of Various diseases and preparation thereof. Patent WO 2009089352, 2009. (9) Mortimore, M.; Young, S. C.; Everitt, S. R. L.; Knegtel, R.; Pinder, J. L.; Rutherford, A. P.; Durrant, S.; Brenchley, G.; Charrier, J. D.; O’Donnell, M. Preparation of 5-cyano-4-(pyrrolo[2,3-b]pyridin-3-yl)pyrimidines as polo-like kinase (PLK) inhibitors. Patent WO2008/79346 , 2008. (10) Ruggeri, S. G.; Hawkins, J. M.; Makowski, T. M.; Rutherford, J. L.; Urban, F. J. Process for preparation of piperidinylaminopyrrolopyrimidines from actiVated pyrrolopyrimidines and piperidinylamines. Patent WO 2007012953 A2, 2007. (11) Heinrich, T.; Blaukat, A.; Staehle, W.; Greiner, H.; Kordowicz, M. NoVel aza heterocycles serVing as kinase inhibitors. Patent WO 2006114180, 2006. (12) Choshi, T.; Yamada, S.; Sugino, E.; Kuwada, T.; Hibino, S. J. Org. Chem. 1995, 60, 5899–5904. (13) Caldwell, J. J.; Cheung, K. M.; Collins, I. Tetrahedron Lett. 2007, 48, 1527–1529. (14) Schneller, S. W.; Luo, J. K. J. Org. Chem. 1980, 45, 4045–4048.

Figure 2. Biarylphosphine ligands and precatalysts.

Figure 1. Pharmacologically active compounds containing the amino-azaindole motif.

reaction of halo-azaindoles with amines. Although azaindoles have previously been reported to undergo arylation of the heterocyclic N-H nitrogen in the presence of copper or palladium catalysts,19,20 the cross-coupling of halo-azaindoles has received little attention.21-23 Haloazaindoles present a particular challenge for two reasons: the donor-acceptor system of the two adjacent nitrogens forms an excellent chelating ligand for metals, and there is the potential for homocoupling between the halide and azaindole N-H. Our recently reported precatalyst systems (Figure 2, P1-P5),24,25 which are efficiently converted to an active monoligated Pd(0) complex when exposed to base, provided a potentially attractive solution to the first problem. We speculated that the preligated palladium species would prove more resistant to undesirable azaindole coordination. To address the second issue of azaindole homocoupling, we hypothesized that the use of a strong base such as LiHMDS, which would fully deprotonate both the amine and azaindole substrates, might reduce the rate of undesired transmetalation to Pd.26 Previous studies in our group support this hypothesis, having demonstrated that the cross-coupling of unprotected (15) Buchwald, S. L.; Mauger, C.; Mignani, G.; Scholz, U. AdV. Synth. Catal. 2006, 348, 23–39. (16) Tasler, S.; Mies, J.; Langa, M. AdV. Synth. Catal. 2007, 349, 2286– 2300. (17) Torborg, C.; Beller, M. AdV. Synth. Catal. 2009, 351, 3027–3043. (18) Carey, J. S.; Laffan, D.; Thomson, C.; Williams, M. T. Org. Biomol. Chem. 2006, 4, 2337–2347. (19) Antilla, J. C.; Klapars, A.; Buchwald, S. L. J. Am. Chem. Soc. 2002, 124, 11684–11688. (20) Old, D. W.; Harris, M. C.; Buchwald, S. L. Org. Lett. 2000, 2, 1403–1406. (21) Guillard, J.; Decrop, M.; Gallay, N.; Espanel, C.; Boissier, E.; Herault, O.; Viaud-Massuard, M. C. Bioorg. Med. Chem. Lett. 2007, 17, 1934–1937. (22) Thibault, C.; L’Heureux, A.; Bhide, R. S.; Ruel, R. Org. Lett. 2003, 5, 5023–5025. (23) Thutewohl, M.; Schirok, H.; Bennabi, S.; Figueroa-Perez, S. Synthesis 2006, 629–632. (24) Biscoe, M. R.; Fors, B. P.; Buchwald, S. L. J. Am. Chem. Soc. 2008, 130, 6686–6687. (25) Fors, B. P.; Watson, D. A.; Biscoe, M. R.; Buchwald, S. L. J. Am. Chem. Soc. 2008, 130, 13552–13554. Org. Lett., Vol. 12, No. 20, 2010

halo-indoles and simple amines could be achieved using LiHMDS as the base, in conjunction with either an XPhos (L3)- or DavePhos (L6)-based catalyst system.27 An examinination of Pd precatalysts based on our biaryl phosphine ligands revealed that cross-coupling between 4-chloroazaindole and N-methylpiperazine occurred rapidly at catalyst loadings as low as 0.5 mol % (Table 1). A

Table 1. Catalyst Systems Used for the Coupling of 4-Chloroazaindole and N-Methylpiperazinea

entry Pd source (mol %) 1 2 3 4 5 6 7 8

P1 (0.5) P2 (0.5) P3 (0.5) P4 (0.5) Pd(OAc)2 (0.5) Pd2dba3 (0.25) Pd(OAc)2 (1) Pd(OAc)2 (1)

ligand (mol %)

time

yield, %

L1 RuPhos (0.5) L2 SPhos (0.5) L3 XPhos (0.5) L4 t-BuXPhos (0.5) L1 RuPhos (1) L1 RuPhos (1) rac-BINAP (2) Xantphos (2)

30 min 30 min 30 min 30 min 30 min 30 min 4h 4h

94 81 90 0 80 33 0 0

a Reagents and conditions: 4-chloroazaindole (0.5 mmol), N-methylpiperazine (0.6 mmol), LiHMDS (1.2 mmol, 1 M in THF).

combination of RuPhos (L1) and RuPhos precatalyst (P1) proved to be the most effective system for this transformation, providing the product in 94% yield after 30 min (Table 1, entry 1), although SPhos (L2) and XPhos (L3) were also effective (Table 1, entries 2 and 3). Interestingly, Pd(OAc)2 can also be employed in lieu of a Pd precatalyst (Table 1, entry 5). However, the rate of formation of Pd(0) from phosphine and Pd(OAc)2 is highly amine-dependent, thus precatalyst P1 was chosen for subsequent studies.28 (26) Biscoe, M. R.; Barder, T. E.; Buchwald, S. L. Angew. Chem., Int. Ed. 2007, 46, 7232–7235. (27) Charles, M. D.; Schultz, P.; Buchwald, S. L. Org. Lett. 2005, 7, 3965–3968. 4439

Alternative base and solvent combinations were also examined (Table 2), as there have been isolated reports of

Scheme 1. Cross-Couplings of 4-Azaindole with Secondary Aminesa

Table 2. Examination of Base and Solvent Combinations for the Cross-Coupling of 4-Chloroazaindolea

entry

base

solvent

temp, °C

time

yield, %

1 2 3 4 5 6 7 8 9

Cs2CO3 NaOt-Bu K3PO4 K2CO3 K2CO3 LiHMDS LiHMDS LiHMDS LiHMDS

toluene toluene toluene toluene tBuOH THF dioxane toluene THF

110 110 110 110 110 65 80 80 rt

16 h 16 h 16 h 16 h 16 h 30 min 4h 4h 16 h

0 7 0 0 0 94b 91b 68b 42b

a

Reagents and conditions: 4-chloroazaindole (0.5 mmol), N-methylpiperazine (0.6 mmol), L1 (1 mol %), P1 (1 mol %), base (1.2 mmol), solvent (1 mL). b L1 (0.5 mol %), P1 (0.5 mol %).

employing NaOt-Bu or Cs2CO3 as base for the cross-coupling reaction of unprotected halo-azaindoles.21-23 We found that procedures using these bases were ineffective with our catalyst systems (Table 2, entries 1-5), with LiHMDS in THF proving optimal in terms of reaction time and temperature. Interestingly, the cross-coupling also proceeded at room temperature (Table 2, entry 9), although longer reaction times and higher catalyst loadings were required for complete conversion. Milder temperatures could be more convenient for parallel reactions or for those involving sensitive substrates. We next applied this Pd-based cross-coupling process to a range of both aliphatic and aromatic secondary amines with 4-chloroazaindole. High yields and selectivities were observed in all cases examined (Scheme 1).29 By the addition of an extra equivalent of LiHMDS, amines containing a second protic functional group could be employed, allowing access to products containing phenols (1b), aliphatic alcohols (1e), or more hindered secondary amines (1c). Not unexpectedly, 4-bromoazaindole displayed reactivity similar to that of its chloro analogue (1b). Without any alteration of the reaction conditions, we also found that 5-bromoazaindole (2a-2f), 6-chloroazaindole (2f), and the related 4-chloro-7H-pyrrolo[2,3-d]pyrimidine (2g) were effective coupling partners with a similarly wide range of secondary amines (Scheme 2). 5-Bromo-3-chloro-7(28) Strieter, E. R.; Buchwald, S. L. Angew. Chem., Int. Ed. 2006, 45, 925–928. (29) In no instance was arylation of the azaindole N-H nor the formation of amino-azaindoles through reaction with LiHMDS observed. 4440

a Reaction conditions: ArX (0.5 mmol), amine (0.6 mmol), L1 (1 mol %), P1 (1 mol %), LiHMDS (1.2 mmol, 1 M in THF). Isolated yields are an average of at least two runs. b L1 (0.5 mol %), P1 (0.5 mol %), 30 min. c 3.6 equiv of LiHMDS.

Scheme 2. Cross-Coupling of 5- and 6-Haloazaindolesa

a Reaction conditions: ArX (0.5 mmol), amine (0.6 mmol), L1 (1 mol %), P1 (1 mol %), LiHMDS (1.2 mmol, 1 M in THF). Isolated yields are an average of at least two runs. b 3.6 equiv of LiHMDS. c L1 (2 mol %), P1 (2 mol %).

azaindole (2h) underwent reaction exclusively at the 5-position, with no diamination or coupling of the chloride observed.30 (30) In the absence of Pd, the halo-azaindoles do not undergo reaction with N-methylpiperazine under the reaction conditions. Org. Lett., Vol. 12, No. 20, 2010

Finally, we explored the cross-coupling of haloazaindoles with primary amines (Scheme 3). We have previously

Scheme 3. Cross-Coupling Using Primary Aminesa

a Reaction conditions: ArX (0.5 mmol), amine (0.6 mmol), L5 (1 mol %), P5 (1 mol %), LiHMDS (1.2 mmol, 1 M in THF). Isolated yields are an average of at least two runs. b No reaction when Pd(OAc)2 (1 mol %) used in place of P5. c Amine purified before use.

reported that catalyst systems based on BrettPhos (L5) are superior to other biarylphosphines for the cross-coupling of primary amines and provide exceptional selectivity for monoarylation.25 Using this system (P5), haloazaindoles

Org. Lett., Vol. 12, No. 20, 2010

underwent efficient cross-coupling with aliphatic, aromatic, and heteroaromatic amines without any other modification of the reaction parameters. While again, in some cases, Pd(OAc)2 can be used as the Pd source, the importance of using the precatalyst (P5) is highlighted in example 3a. In cases where the reacting amine lacks a β-hydrogen atom, Pd(OAc)2 cannot be reduced, and thus no cross-coupling occurs. We also found that the addition of extra ligand is not always necessary. For example, 3a was isolated in a yield of 88% in both the presence or absence of an extra equivalent of BrettPhos (L5). In summary, we have developed operationally simple and efficient methods for the cross-coupling of unprotected halo7-azaindoles with a wide range of primary and secondary amines. Notably this reaction can be performed in the presence of a variety of protic functional groups. The success of these reactions further demonstrates the advantages of conducting Pd-catalyzed cross-coupling reactions using metallacyclic precatalysts such as P1 and P5, as these precatalysts permit rapid Pd activation in the presence of a wide range of substrates. Acknowledgment. This work is supported by an educational donation provided by Amgen and from the National Institutes of Health Grant (GM-58160) to whom we are grateful. Supporting Information Available: Experimental procedures and spectral data for all products. This material is available free of charge via the Internet at http://pubs.acs.org. OL101928M

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